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Multiple Myeloma | Cancer of the Bone Marrow
Concise
Review
of the Disease
and Treatment Options
2015 Edition | Prepared by Brian G.M. Durie, MD
A publication of the International Myeloma Foundation
Improving Lives Finding the Cure®
About the International Myeloma Foundation
Founded in 1990, the International Myeloma Foundation (IMF) is the
oldest and largest myeloma-specific charity in the world. With more than
350,000 members in 140 countries, the IMF serves myeloma patients, family
members, and the medical community. The IMF provides a wide range of
programs in the areas of Research, Education, Support, and Advocacy:
RESEARCH The IMF is the leader in globally collaborative myeloma research.
The IMF supports lab-based research and has awarded over 100 grants to top
junior and senior researchers since 1995. In addition, the IMF brings together
the world’s leading experts in the most successful and unique way through the
International Myeloma Working Group (IMWG), which is publishing in prestigious
medical journals, charting the course to a cure, mentoring the next generation
of innovative investigators, and improving lives through better care.
EDUCATION The IMF’s educational Patient & Family Seminars, Medical Center
Workshops, and Regional Community Workshops are held around the world.
These meetings provide up-to-date information presented by leading myeloma
specialists and researchers directly to myeloma patients and their families.
Our library of more than 100 publications, for patients and caregivers as well as
for healthcare professionals, is updated annually and available free of charge.
Publications are available in more than 20 languages.
SUPPORT Our toll-free InfoLine at 800-452-CURE (2873) is staffed by
coordinators who answer questions and provide support and information
via phone and email to thousands of families each year. The IMF sustains a
network of more than 150 support groups and offers training for the hundreds
of dedicated patients, caregivers, and nurses who volunteer to lead these
groups in their communities.
ADVOCACY The IMF Advocacy program trains and supports concerned
individuals to advocate on health issues that affect the myeloma community.
Working both at the state and federal level, the IMF leads two coalitions to
advocate for parity in insurance coverage. Thousands of IMF-trained advocates
make a positive impact each year on issues critical to the myeloma community.
Learn more about the way the IMF is helping to improve the quality of life
of myeloma patients while working toward prevention and a cure.
Contact us at 800-452- CURE (2873) or visit myeloma.org.
Improving Lives Finding the Cure®
Table of contents
Introduction
4
What is myeloma?
4
Production of monoclonal protein by myeloma cells
4
Annotated history
5
Epidemiology
11
Pathophysiology
11
Bone disease
11
Anemia
12
Kidney dysfunction
12
Other organ dysfunction
13
Types of myeloma
13
Clinical symptoms
13
Staging and prognostic factors
14
Definition of clinical response
17
Treatment
17
Options for patients who are not candidates for transplant
19
Transplantation
21
Radiation
24
Maintenance therapy
25
Supportive care
25
Management of relapsing or refractory disease
27
New and emerging treatments
29
References
29
Introduction
The IMF Concise Review of the Disease and Treatment
Options is an overview of myeloma, with a discussion of pathophysiology, clinical features, and
treatment options. We hope that the information
will be helpful to both healthcare professionals
and patients.
What is myeloma?
Myeloma is a cancer of the plasma cells in the bone
marrow. Myeloma is synonymous with “multiple
myeloma” and “plasma cell myeloma.” The malignant plasma cells (see Figure 1), or myeloma cells,
accumulate in the bone marrow. The major features
of myeloma result from the abnormal accumulation
of myeloma cells within the bone marrow, causing:
—
Disruption of normal bone marrow function
reflected by anemia and/or low white counts or
platelet counts;
— Destruction and invasion of bone and surrounding areas of bone marrow involvement;
— Production and release of monoclonal protein
from the myeloma cells into the blood stream
and/or into the urine;
— Reduction of normal immune function, reflected
by reduced levels of normal immunoglobulins
and increased susceptibility to infection. Infection is also more likely if the white blood cell
count is low.
Production of monoclonal
protein by myeloma cells
The characteristic property of myeloma cells is
the production and secretion (release) of monoclonal protein into the blood and/or urine. The
amount of monoclonal protein produced by
myeloma cells varies considerably from patient to
patient. In assessing myeloma, it is very important
to know if a patient’s myeloma cells are high producers or low producers or non-secretors (with
no protein released into the blood or urine). Once
the relationship between the protein level and the
amount of myeloma in the bone marrow is known,
it is possible to interpret and understand the relationship between a particular protein level and the
myeloma tumor burden. Monoclonal protein is also
called M-protein, M-component, myeloma protein,
paraprotein, protein spike, or M-spike. The monoclonal protein is called a spike because of the way
it appears on protein electrophoresis, a laboratory
technique used to separate and identify proteins
(see Figure 2).
Figure 2. Monoclonal Spike
Figure 1. Myeloma Cells
Myeloma cells producing M-protein
Plasmacytomas are localized tumors composed of
plasma cells, which can grow inside bone (intramedullary) or outside bone (extramedullary or
soft-tissue). When there are multiple plasmacytomas inside or outside bone, this condition is
also called multiple myeloma. When patients with
myeloma have disease outside the bone marrow,
this is called “extra medullary disease” (EMD).
4
The monoclonal protein is an immunoglobulin
or a component/fragment of an immunoglobulin.
Figure 3 illustrates the structure of a normal immunoglobulin molecule. In myeloma cells, mutations
have occurred in the genes responsible for immunoglobulin production. Myeloma proteins therefore have an abnormal amino acid sequence and
protein structure. Typically, the normal antibody
function of the immunoglobulin is lost, and the
three-dimensional structure of the molecule may
be abnormal.
Increased production of abnormal immunoglobulin has a number of consequences:
800-452-CURE (2873)
—E
xcess monoclonal protein accumulates in the
bloodstream and/or is excreted in the urine.
Figure 3. Immunoglobulin Molecule Structure
—
The abnormal monoclonal molecules can
adhere to each other and/or to other tissues
such as blood cells, blood vessel walls, and other
blood components. This can reduce blood flow
and circulation, causing hyperviscosity syndrome
(discussed in text).
— Approximately 30% of the time, more light
chains are produced than are needed to combine with the heavy chains to create a whole
immunoglobulin molecule. These excess light
chains are called Bence Jones proteins (see “Annotated history” section). Free Bence Jones proteins
have a molecular weight of 22,000 daltons and
are small enough to pass freely into the urine.
—T
he abnormal monoclonal proteins can also
have a wide range of other properties including:
Binding to normal blood clotting factors,
¡
resulting in increased bleeding tendency,
enhanced blood clotting, or phlebitis (inflammation of the veins);
Binding to nerves to cause neuropathy or
¡
to circulating hormones to cause metabolic
dysfunction.
— Free Bence Jones proteins can also adhere
to each other and/or to other tissue (just as the
whole immunoglobulin molecule can). In this
case the end result is either:
1. A
L Amyloidosis – Disease in which the Bence
Jones light chains (usually lambda) are crosslinked in a highly symmetric “beta-pleated”
fashion and become deposited in tissue
around the body, including, for example, kidney, nerves, and heart tissue; or
2. L
ight Chain Deposition Disease (LCDD) –
Light chains (usually kappa) are deposited in a
more haphazard fashion, but most selectively in
small blood vessels of the eyes and kidneys; or
3. M
onoclonal Immunoglobulin Deposition
Disease (MIDD) – Disease in which there is
deposition of fragments of heavy chains, light
chains, or both heavy and light chains.
It is important to be aware that routine blood testing can give very strange results because of “stickiness” or hyperviscosity of myeloma blood samples
in automated chemical analyzers and/or interference with chemical reactions.
myeloma.org
Annotated history
Dr. Henry Bence Jones was the first to investigate
a strange protein in the urine of a patient with
myeloma. What caught his attention was a urine protein that dissolved on boiling, but re-precipitated on
cooling: these are called “Bence Jones” light chains.
This patient also had a strange bone disease that we
now call multiple myeloma. The following is a brief
annotated summary of progress in research and
treatment for myeloma and related diseases from
that time forward.
1844–1850
First case descriptions of myeloma referred to as
“mollities and fragilitas ossium” (soft and fragile
bones). The first documented patient, Thomas
Alexander McBean, was diagnosed in 1845 by
Dr. William Macintyre in London. The unusual urine
problem he discovered was fully investigated by
Dr. Henry Bence Jones, who published his findings
in 1848. In 1846, Mr. John Dalrymple, a surgeon,
determined that the diseased bones contained cells
subsequently shown to be plasma cells. Dr. Macintyre published the full details of this case of Bence
Jones myeloma in 1850. Dr. Samuel Solly published
a similar case of myeloma (Sarah Newbury) in 1844,
but without any detailed urine studies.
1873
Von Rustizky introduced the term “multiple
myeloma” to designate the presence of multiple
plasma cell lesions in bone.
1889
Otto Kahler published a detailed clinical description of multiple myeloma, “Kahler’s disease.”
5
1890
1969
Ramon y Cajal provided the first accurate microscopic description of plasma cells.
Melphalan combined with prednisone was shown
by Alexanian to produce better results than melphalan alone.
1900
J.H. Wright discovered that myeloma cells are
plasma cells.
1903
Weber noted that myeloma bone disease (lytic
lesions) is detectable using x-rays.
1909
Weber suggested that plasma cells in the bone
marrow cause the myeloma bone destruction.
1930s
The routine diagnosis of myeloma remained difficult until the 1930s, when bone marrow aspirates
were first used on a larger scale. The development
of the ultracentrifuge and serum/urine protein
electrophoresis improved both screening and
diagnosis.
1953
Immunoelectrophoresis allowed exact identification of the monoclonal myeloma proteins. Immunofixation has since been introduced as a more
sensitive method.
1975
Durie-Salmon Staging System for myeloma introduced. Patients classified to assess benefits of
chemotherapy at different disease stages (I, II, III, A
or B).
1976–1992
Various combinations of chemotherapy agents
tried, including the M2 regimen (VBMCP), VMCPVBAP, and ABCM, with some indication of superiority versus MP. However, in 1992, a comparative
meta-analysis (Gregory) showed equivalent results
for all combinations.
1979–1980
Labeling index (growth fraction analysis) first introduced as a test in myeloma and related diseases.
Stable remission or plateau phase of myeloma identified. Plateau phase is a period when the growth
fraction (LI%) of residual bone marrow plasma cells
is zero.
1956
1982
Korngold and Lipari noted that Bence Jones proteins are related to normal serum gamma globulin
as well as abnormal serum proteins. In their honor,
the two types of Bence Jones proteins are called
kappa (ĸ), and lambda (λ).
Twin transplants performed by Fefer and Osserman
as treatment for myeloma.
1983
1958
1984
Discovery of sarcolysin in the USSR. From this, melphalan (Alkeran®) was derived. For the first time,
treatment was possible.
1961
Waldenström emphasized the importance of the
differentiation between monoclonal and polyclonal gammopathies. He associated IgM monoclonal proteins with macroglobulinemia as distinct
from myeloma.
First use of serum β2 microglobulin as a prognostic
test (Bataille, Child, and Durie).
Barlogie and Alexanian introduce VAD (vincristine/
Adriamycin/dexameth­asone) chemo­therapy.
1984–1986
First reports of allogeneic transplants in myeloma
by various investigators.
1986–1996
First report of successful treatment of myeloma
with melphalan by Bergsagel.
Large numbers of studies evaluating high-dose
therapy with autologous bone marrow or stem
cell rescue by various investigators. Both single
(McElwain) and double (Barlogie) transplant procedures introduced.
1964
1996
1962
First report of successful treatment of myeloma
with cyclophosphamide (Cytoxan®) by Korst.
Results with cyclophosphamide proved to be similar to results with melphalan.
6
— First randomized study indicating possible benefit of high-dose therapy with bone marrow transplant support versus standard chemotherapy
(Attal on behalf of IFM group).
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— Randomized study of the bisphosphonate pamidronate (Aredia®) versus placebo indicates reduction in bone problems (“skeletal related events”).
2001
1997
2002
Evidence that viruses may be involved in triggering
myeloma. Myeloma more common in patients with
HIV and hepatitis C. Human herpes virus-8 (HHV-8)
found in bone marrow dendritic cells. RNA found
in blood with specificity for SV40 cancer-causing
monkey virus.
— Evidence of efficacy of new agents in clinical trials including Velcade (Phase III, Millennium) and
Revlimid (Phase III, Celgene).
— Thalidomide combined with dexamethasone as
frontline therapy for myeloma produces response
rate of approximately 70%.
1998
— In the United Kingdom, Medical Research Council
(MRC) reports autotransplant results at American
Society of Hematology (ASH) annual meeting.
Overall benefit noted, especially for patients with
high serum β2 microglobulin (> 7.5 mg/L).
— Continued research on the role of high-dose
chemotherapy with autologous and allogeneic
transplant. The magnitude of benefit and patient
population(s) likely to benefit remain uncertain.
Transplant performed as part of initial (induction)
therapy is shown to produce results similar to
transplant done at first relapse.
— Chromosome 13 deletions shown to be poor
prognostic factor for transplantation as well as
some other therapies.
— New study reconfirms prednisone as a helpful
maintenance therapy with prolongation of remission. Alpha interferon also shown again to have
some benefit in prolonging remission.
1999
— Thalidomide shown to be an effective anti-myeloma therapy in patients with relapsing/refractory disease.
— Mini-allogeneic transplant introduced as less
toxic method to achieve a graft-versus-myeloma
effect.
— Randomized French study shows no major benefit of double autologous transplant versus single
transplant.
— Longer-term follow-up shows that Aredia treatment continued for 2 years is helpful.
2000
For the first time, there are several promising new
approaches for myeloma therapy. New clinical trials
include thalidomide analogues (e.g., lenalidomide
or Revlimid®), long-acting Adriamycin® analogues
(e.g., pegylated doxorubicin or Doxil®), arsenic
trioxide (Trisenox®), anti-angiogenesis agents
(e.g., VEGF tyrosine kinase inhibitor), agents to
block cell adhesion, and proteasome inhibitors
(e.g., bortezomib or Velcade®).
myeloma.org
New classification system proposed for myeloma
and related diseases
2003
— Bortezomib (PS-341 or Velcade) approved in the
United States by the Food and Drug Administration (FDA) as treatment for relapsed myeloma
following at least two prior therapies.
— MRC autotransplant results provide the second
randomized data set indicating benefit of autotransplant versus standard-dose chemotherapy.
— Results of Intergroupe Francophone du Myélome
(IFM) study comparing single with double transplant shows overall benefit with the double transplant after more than four years of follow-up.
However, no apparent added benefit is shown for
patients already in complete remission with the
first transplant.
— Little Rock group (Shaugnessy/Barlogie) shows
that bone disease in myeloma is associated with
production of a particular protein called DKK-1.
2004
— Results of ECOG randomized trial comparing thalidomide plus dexamethasone versus dexamethasone alone for previously untreated myeloma
indicate a 59% response rate with the combination versus 41% with dexamethasone alone
(ECOG Criteria).
— Results of multi-institutional randomized trial
comparing Velcade with dexamethasone show
superiority of Velcade (discussed in text).
— Early results with Velcade in the frontline setting
show excellent results: 83% response rate with
Velcade/dexamethasone and 94% with Velcade/
7
Adriamycin/dexamethasone and the ability to
harvest stem cells with successful transplantation
and engraftment.
— New myeloma staging system introduced, the
International Staging System (ISS).
2005
— Two large Phase III trials show that lenalidomide
plus dexamethasone is superior to dexamethasone alone in relapsed myeloma (time to progression > 15 months versus 5 months).
— Velcade receives full FDA approval for treatment
of patients with myeloma after 1 prior therapy.
— International Staging System (ISS), developed
by the International Myeloma Working Group
(IMWG) of the International Myeloma Foundation
(IMF), is published (see Table 5).
— Numerous new agents in early development.
— Addition of thalidomide to standard melphalan/
prednisone regimen shows remarkable added
benefit. Several upfront trials are ongoing.
2006
— New response criteria for assessing treatment
benefit are developed and published.
— Lenalidomide (Revlimid) receives FDA approval
for treatment of myeloma in combination with
dexamethasone in patients who have received at
least 1 prior therapy.
— Numerous new agents continue to be developed.
2007
— FDA accepts a supplemental NDA for use of Velcade plus Doxil to treat relapsed or refractory
myeloma in patients who have not previously
received Velcade and have received at least 1
prior therapy.
— Combination thalidomide/dexamethasone plus
Doxil compared with thalidomide/dexamethasone
in a Phase III trial for newly diagnosed myeloma.
2008
— Thalidomide approved by the European Medicines Agency (EMA) as part of the MPT regimen
(melphalan/prednisone/thalidomide) for frontline therapy.
— Velcade approved by the FDA as part of the VMP
regimen (Velcade/melphalan/prednisone) for
frontline therapy.
8
— Many new drugs in development and trials ongoing. The second-generation proteasome inhibitor
carfilzomib (PR-171 or Kyprolis®) shows promise
in early trials.
— FDA approves plerixafor (Mozobil®) in combination
with G-CSF for collection of stem cells for autologous transplantation in patients with myeloma.
2009
— Development of new drugs continues, including
encouraging results from trials of second-generation proteasome inhibitors Kyprolis and NP-0052;
HDAC inhibitors vorinostat and panobinostat;
HSP-90 disrupter tanespimycin; monoclonal
antibody elotuzumab; and third-generation
immunomodulatory drug (IMiD®) pomalidomide
(Pomalyst®).
— IMWG analysis shows cytogenetic and FISH abnormalities combined with ISS stage are prognostic;
some novel therapies overcome poor risk factors.
— Positive results with CyborD induction therapy for
newly diagnosed myeloma.
— IMWG publishes guidelines for serum free light
chain analysis as well as consensus statement and
guidelines for imaging techniques in the diagnosis and monitoring of myeloma.
— Several publications by Landgren support genetic
features in pathogenesis of monoclonal gammopathy of undetermined significance (MGUS),
and Weiss demonstrates that an MGUS precedes
myeloma in most patients.
2010
— FDA approves a risk evaluation and mitigation
strategy (REMS) to ensure the safe use of erythropoiesis-stimulating agents (ESAs), which may
promote tumor growth, shorten survival, and
increase the risk of cardiovascular adverse events.
— Preliminary identification of erythropoietin (Epo)
receptors on myeloma cells.
— Development of new drugs continues, including more encouraging results from trials of second-generation proteasome inhibitor Kyprolis;
HDAC inhibitors vorinostat and panobinostat;
monoclonal antibody elotuzumab; and third-generation IMiD Pomalyst.
— Several studies suggest a role for lenalidomide
maintenance therapy.
— Frontline therapy with novel agents may be as
effective as transplantation in eligible patients.
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— Zoledronic acid (Zometa®) may have an antimyeloma effect; effective dental hygiene has
reduced occurrence of osteonecrosis of the jaw
(ONJ).
— Rajkumar demonstrates superiority of lenalidomide plus low-dose dexamethasone over lenalidomide plus standard-dose dexamethasone in
ECOG E4A03 trial.
— Richardson publishes positive results with induction therapy for newly diagnosed myeloma with
RVD (Revlimid/Velcade/dexamethasone).
— IMWG publishes consensus statement on allogeneic transplant, recommending that it be done
for myeloma patients only within the context of
a clinical trial.
2011
— Approval of subcutaneous (SQ) administration of
Velcade based on international Phase III trial led
by Moreau (IFM group).
— San Miguel and Landgren articulate the need to
redefine asymptomatic or smoldering multiple
myeloma (SMM) and to treat high-risk SMM.
— Palumbo publishes new paradigm for the treatment of older patients.
— Landgren and National Cancer Institute (NCI)
team demonstrate higher incidence of MDS and
AML among patients with MGUS.
— CAFE study demonstrates that balloon kyphoplasty is superior to non-surgical approaches in
management of painful vertebral compression
fractures.
— Complete response (CR) after stem cell transplant
determined to be a “central prognostic factor” by
Spanish Myeloma Group (GEMM).
— Italian group demonstrates correlation of CR with
long-term PFS and OS in elderly patients treated
with novel agents.
— IMWG publishes guidelines for the treatment of
patients who are candidates for autologous stem
cell transplant.
2012
— Carfilzomib (Kyprolis) receives FDA approval for
the treatment of patients with myeloma who have
had at least two prior therapies, including bortezomib and an IMiD, and demonstrated disease progression on or within 60 days of the last therapy.
myeloma.org
— IMWG publishes data on progression and survival
after treatment with IMiDs and bortezomib, and
establishes a benchmark of 9-month median OS.
— IMWG publishes consensus statement on
plasma cell leukemia, including diagnostic
requirements, response criteria, and treatment
recommendations.
— 4-drug EVOLUTION study with bortezomib, dexamethasone, cyclophosphamide, and lenalidomide demonstrates no benefit and more toxicity
than 3-drug regimens VCD and VDR.
— Faham presents paper on detection of circulating myeloma cells in the peripheral blood of
93% of the patients tested with high-throughput
sequencing of DNA and RNA.
— Studies of carfilzomib in combination therapies
(KCyD, KRD, KTD, KCyTD) and of pomalidomide
in combination therapies (Pd, PKD, PCyPred,
BiaxinPD, PcyD, PVDd) demonstrate their efficacy
as “platform” drugs.
— First studies of oral proteasome inhibitors,
MLN9708 (ixazomib) and ONX0912 (oprozomib).
— First studies of anti-CD 38 monoclonal antibody,
daratumumab, demonstrate single-agent activity.
2013
— Pomalidomide (Pomalyst) receives FDA approval
for patients with myeloma who have received at
least two prior therapies including lenalidomide
and bortezomib and have demonstrated disease
progression on or within 60 days of completion of
the last therapy.
— First studies presented of anti-CD monoclonal
antibody, SAR650984, demonstrate single-agent
activity.
— Mateos et al. publish results of trial comparing
lenalidomide plus dexamethasone versus observation in high-risk SMM. Time to progression
(TTP) and overall survival (OS) significantly longer
in the lenalidomide/dexamethasone arm.
— IFM’s FIRST trial demonstrates superiority of continuous lenalidomide/dexamethasone over MPT
or lenalidomide/dexamethasone for 18 months,
laying the groundwork for later EMA approval of
frontline lenalidomide.
— Combination of bortezomib, dexamethasone,
and HDAC inhibitor panobinostat for relapsed/
refractory myeloma improves progression-free
survival over bortezomib/dexamethasone.
9
— Two studies determine that progression of SMM
to active disease is significantly different based
on the underlying cytogenetic subtype of the
disease.
— Paiva et al. publish an immunophenotypic algorithm to identify newly diagnosed myeloma with
an MGUS-like signature and long-term disease
control.
— Dispenzieri et al. reclassify highest-risk SMM as
active MM requiring treatment.
— Palumbo et al. determine that continuous therapy improves PFS1, PFS2, and OS over fixedduration therapy.
— Hevylite® test approved by FDA for use in IgA and
IgG myeloma.
— Russell publishes proof of principle on systemic
oncolytic virotherapy with measles virus.
— IMWG publishes updated criteria for the diagnosis of myeloma, defining ultra-high-risk SMM as
myeloma.
2014
2015
— Palumbo publishes meta-analysis of second primary malignancies with lenalidomide therapy
and identifies increased risk with combination
of melphalan/lenalidomide, but not with lenalidomide/cyclophosphamide or lenalidomide/
dexamethasone.
— Drake et al. find that cortical microarchitecture is
weakened in MGUS patients compared to agematched controls.
— New methods of minimal residual disease (MRD)
detection by multiparameter flow cytometry and
deep sequencing provide higher sensitivity in
quantifying response to treatment.
— FDA approves use of Spanish flow MRD evaluation as a new end-point in myeloma clinical trials.
— FDA approves lenalidomide (Revlimid) in the
frontline setting based on the FIRST trial, with
caveats about harvesting stem cells after only
four cycles of therapy, careful monitoring of
blood counts, and risk of SPMs in the post-transplant setting.
— IMWG publishes report on geriatric assessment
tool developed by Palumbo et al.
— IMWG publishes consensus statement on the
role of MRI in the management of patients with
myeloma.
— FDA approves panobinostat (Farydak®) in combination with bortezomib and dexamethasone for
the treatment of patients with multiple myeloma
who have received at least two prior regimens,
including bortezomib and an IMiD.
Table 1. Definitions of MGUS and Myeloma
NAME
DEFINITION
Monoclonal Gammopathy
of Undetermined Significance
(MGUS)
Smoldering Multiple Myeloma
(SMM)
• Monoclonal protein present but usually < 3.0 g/dL
• No CRAB features or other indicators of active myeloma
• Bone marrow monoclonal plasma cells < 10%
• Higher level of disease than MGUS: serum M-component can be > 3.0 g/dL
and/or bone marrow plasma cells between 10% and 60%, but
• No CRAB features or other indicators of active myeloma
• > 60% bone marrow plasma cells
• Free light chain ratio >100
• >1 MRI focal lesion
• Monoclonal protein present, and
• One or more “CRAB” features and/or indicators of organ damage*
Early Active Myeloma
Active Myeloma
*Organ damage classified as “CRAB” or any other significant clinical problem linked to myeloma progression
such as recurrent infections or neuropathy unrelated to treatment
C – calcium elevation (> 10 mg/dL)
R – renal dysfunction (creatinine > 2 mg/dL or creatinine clearance <40 ml/min)
A – anemia (hemoglobin < 10 g/dL or > 2g/dL decrease from patient’s normal)
B – bone disease (one or more osteolytic lesions detected on skeletal radiography, WBLC CT, or PET/CT)
One or more “CRAB” features or other significant problem required for diagnosis of Symptomatic Myeloma
10
800-452-CURE (2873)
Epidemiology
The average incidence of myeloma is 3-4/100,000
in the US, representing approximately 1.3% of all
types of cancer. According to the American Cancer Society, an estimated 26,850 Americans will be
diagnosed with myeloma in 2015, and an estimated
11,240 people will die from the disease. There are
currently approximately 88,490 Americans living
with the disease. Myeloma is more common in
African-Americans than Caucasians. For example,
in Los Angeles County, the incidence of myeloma
in African-American men is 9.8/100,000, versus
4.3/100,000 for Caucasian men. The incidence varies
from country to country from a low of < 1/100,000
in China to approximately 4/100,000 in most industrialized Western countries. The male:female ratio
is 1.25:1 in the US. Incidence of myeloma rises with
age. Better diagnostic techniques and the higher
average age of the general population may, in part,
explain the rising incidence over the last several
decades. A trend toward more frequent myeloma
in patients under age 55 implies important environmental causative factors in the past 60 years. Several recent studies have evaluated the causation of,
or predisposition to, myeloma, MGUS, and related
disorders. Environmental or work-related exposures to toxic chemicals are definite causal factors.
Firefighters, other first responders, and individuals
in a variety of other occupations with toxic exposure such as farmers and farm-workers, as well as
individuals who are obese, are at increased risk
of myeloma. Eating seafood contaminated with
heavy metals and/or chemicals may be a risk factor
for myeloma. Other medical conditions including
immune system disorders and infections can be
underlying and/or trigger factors. Several studies
are focused on the genetic risk factors for myeloma.
Pathophysiology
The uncontrolled growth of myeloma cells has
many consequences, including:
— skeletal destruction;
— bone marrow failure;
— increased plasma volume and viscosity;
— suppression of normal immunoglobulin
production;
— renal insufficiency.
myeloma.org
Nonetheless, the disease can remain asymptomatic
for many years, as noted in the discussion of MGUS.
In the symptomatic phase, the most common presenting complaint is bone pain. The serum and/or
urine M-protein is elevated and typically rising at
the time of diagnosis. (Please note: “M” is used for
Monoclonal, Myeloma, Monoclonal immunoglobulin, and M-component. These are not quite identical, but are used synonymously.) The overall pattern
of disease phases for patients with myeloma is illustrated in Figure 4. It is important to note that there
can be multiple periods of response and remission.
The pathophysiology of myeloma is summarized in
Table 2 in schematic form.
Figure 4. Disease Phases
Bone disease
Ever since the first recognition of myeloma in 1844,
there has been awareness of an unusual and unique
type of bone disease. It has taken until quite recently
to determine the mechanisms involved. The first
clue was that both myeloma cells and increased
numbers of osteoclasts are present at sites of bone
destruction. Understanding of the mechanisms has
evolved from the observation that myeloma cells
produce osteoclast-activating factors (OAFs) to the
identification of local cytokines such as IL-1β, IL-6,
and TNF-α and -β; chemokines such as MIP-α, and
cell-cell adhesion processes involving β3 integrin,
all of which are involved in producing increased
numbers and activity of osteoclasts. A substance
called RANK ligand (RANKL) has been identified as
a critical mediator of osteoclast activation. Many
details of the mechanisms of bone disease in
myeloma are now understood. Several targets for
treatment approaches have been identified.
Besides activation of osteoclasts, the other characteristic feature of myeloma bone disease is inhibition
11
Table 2. Schema of Pathophysiology
Skeletal Findings
• Solitary or multiple osteolytic lesions
• Diffuse osteoporosis (osteopenia)
Associated Effects of
Bone Destruction
• Elevated serum calcium
• Hypercaliuria (calcium increase in urine)
• Bone fractures
• Loss of height (vertebral collapse)
Extramedullary Myeloma • Soft tissue involvement, mostly common in head/neck area (e.g. nasopharynx);
also in liver, kidney, and other soft tissue sites including skin
(extraskeletal)
Peripheral Blood
• Anemia
• Abnormal clotting
• Leukopenia
Plasma Protein Changes
• Hyperproteinemia (elevated protein)
• Hypervolemia (expanded volume)
• Monoclonal immunoglobulins
(IgG, IgA, IgD, IgE, IgM or light chains only)
• Narrowed anion gap (low serum sodium)
• Elevated serum β2-microglobulin
• Decreased serum albumin
• Elevated serum IL-6 and C-reactive protein (CRP)
Kidney Abnormalities
• Proteinuria, casts without leukocytes
or erythrocytes
• Tubular dysfunction with acidosis
(Fanconi syndrome)
• Uremia (kidney failure)
• Amyloidosis or light chain deposition disease
and renal dysfunction
• Thrombocytopenia
• Circulating monoclonal B lymphocytes
(precursors of myeloma cells)
• Plasma cell leukemia
• Circulating plasma cells
of osteoblasts, which are responsible for new bone
production and bone healing. “Coupling” between
osteoclast and osteoblast function is responsible
for normal bone remodeling and repair. The mechanisms responsible for “un-coupling” in myeloma
are also under investigation. An important new
observation is that the cholesterol-lowering statins
(HMG-CoA reductase inhibitors, e.g., Lipitor®, Mevacor®) can enhance osteoblast activity and promote
bone healing. Both bortezomib and lenalidomide
have been shown to promote bone healing in
addition to exerting potent anti-myeloma activity.
Studies to further investigate the benefit of several
new bone therapies are ongoing.
Anemia
Anemia is a characteristic feature of myeloma.
Although simple physical displacement of marrow
red blood cell precursors is undoubtedly a factor,
the specific inhibition of red cell production by
micro-environmental cytokine and adhesion molecule effects is a more functional explanation. Two
research teams have described the involvement
of hepcidin (a peptide hormone that controls iron
regulation) in anemia caused by myeloma. Their
research was based on the hypothesis that interleukin-6 (IL-6) and certain bone morphogenetic proteins (BMPs), cytokines produced in myeloma, are
12
also known to be regulators of hepcidin. Improvement in anemia thus occurs with successful treatment of the myeloma. Recombinant Epo (e.g.,
Epogen® or Procrit®) should be used with caution
in the light of reports of the association of Epo with
increased tumor growth and reduced survival in
patients with cancer, and the identification of Epo
receptors on myeloma cells.
Kidney dysfunction
Impairment of kidney function is a common complication in patients with myeloma. However, this
does not mean that every patient will have this
problem. In some patients, myeloma proteins, especially Bence Jones light chains, cause renal injury by
a variety of mechanisms ranging from tubular damage resulting from large accumulations of precipitated light chains, to effects of myeloma proteins
deposited as amyloid, to selective tubular damage
resulting in the metabolic effects of an entity called
Fanconi syndrome. Fanconi syndrome is a type of
selective kidney tubular damage with leakage of
amino acids and phosphates into the urine, which
can in turn cause metabolic bone disease.
Other important factors related to kidney dysfunction in myeloma patients are increased levels of calcium and/or uric acid, infection, and the effects of
drugs such as nephrotoxic antibiotics, nonsteroidal
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anti-inflammatory drugs (NSAIDS), or contrast
agents or dyes used for diagnostic studies. An
important observation is the potentially toxic effect
of gadolinium-based contrast agents used with
MRI. Patients with kidney problems should discuss
the use of gadolinium with their physicians. Awareness of potential kidney damage and maintaining
sufficient fluid intake are especially important for
patients with myeloma to help avert the damaging
effects of these various factors.
Other organ dysfunction
Myeloma cells can accumulate in bone marrow
and/or in a variety of tissue sites and produce a
broad range of potential complications.
— Neurologic Effects – Nerve tissue is often
affected in myeloma patients either by the direct
antibody effects of myeloma proteins against
nerves (e.g., myelin sheaths) or by deposition of
amyloid fibrils on nerves, thus impairing function.
These effects result in peripheral neuropathies
that must be distinguished from other causes of
neuropathy such as diabetes mellitus, or from primary nerve disorders such as multiple sclerosis,
Parkinson’s disease, and many others. Because
of myeloma patients’ susceptibility to infection,
viral infections of nerve tissue are quite common,
most particularly varicella zoster (shingles), herpes zoster (cold sores), Epstein-Barr virus (mononucleosis), or cytomegalovirus, which may result
in Bell’s Palsy (partial facial paralysis) or other
complications.
— Plasmacytomas – Both in bone and in soft tissue, plasmacytomas can result in compression or
displacement of nerves, the spinal cord, or even
brain tissue. These pressure effects often represent a medical emergency and require immediate treatment with high doses of corticosteroids,
radiation therapy, or neurosurgery.
— Infections – The predisposition to infections is
perhaps the single most characteristic feature of
myeloma patients besides the strong tendency
for bone disease. The mechanisms responsible for infection susceptibility are not fully
understood. The presence of active myeloma
in the bone marrow results in impairment of
normal immune function, including inhibition
of normal antibody production (reflected by
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hypogammaglobulinemia), impaired T-lympho­
cyte function, and activated but aberrant
monocyte/macrophage function. Some studies
indicate that a factor issuing from the activated
macrophages both enhances the activity of the
myeloma and inhibits normal immunoglobulin
production and T-lymphocyte function.
Myeloma patients are susceptible to both viral
infections and infections with “encapsulated”
bacteria such as pneumococcus. However, in the
face of neutropenia and the effects of high-dose
chemotherapy, and with the added local effects of
implanted catheters (e.g., Hickman and Groshon
catheters or PICC lines), the whole range of bacterial, fungal, and opportunistic infections can occur
in patients with myeloma undergoing therapy.
In summary, key aspects of infections in
myeloma patients are:
— Reduced immunity because of myeloma
—
Low white blood cell counts because of
myeloma build-up in bone marrow and/or the
impact of treatment.
Infection, or any question of infection, should
not be ignored. Prompt review is required to
assess the need for immediate antibiotic and/or
antiviral therapy. Many patients learn to have therapy on hand for any emergency.
Types of myeloma
The type of monoclonal protein produced varies
from patient to patient. The most common is IgG
and the least common is IgE. Table 3 shows the
percentages of different types of myeloma. Each
type is associated with slightly different patterns
of disease. For example, IgA myeloma is more commonly associated with disease outside bone (extramedullary disease), whereas IgD myeloma is more
commonly associated with plasma cell leukemia
and renal damage.
Clinical symptoms
About 70% of patients with myeloma present with
pain of varying intensity, often in the lower back or
ribs. Sudden severe pain can be a sign of fracture or
collapse of a vertebral body. General malaise and
vague complaints are frequent. Significant weight
loss is rare.
13
Table 3. Types of Monoclonal Protein (%)*
%
Totals
1. Serum
IgG
52
IgA
21
IgD
2
IgE
< 0.01
75%
2. Urine (Bence Jones or light chains only)
types κ and λ
11%
3. Two or more
monoclonal paraproteins
<1
Heavy chains (G or A) only
<1
No monoclonal paraprotein
2%
1
4. IgM (rarely myeloma typically associated
with Waldenström’s macroglobulemia)
Total
12%
100%
* This includes different types of MGUS and myeloma
as well as Waldenström’s macroglobulemia.
Source: Data on 1,827 myeloma patients collected and
analyzed by Pruzanski and Ogryzlo, 1970.
Both neutropenia and hypogammaglobulinemia
(immunoparesis) increase the likelihood of infections. Although pneumococcal pneumonia is the
classic infection associated with myeloma at presentation, other bacteria, such as streptococci and
staphylococci, are now frequently isolated. Haemophilus infection and herpes zoster infections
also occur.
Hypercalcemia, historically found in 30% of patients
at diagnosis, causes tiredness, thirst, and nausea.
Precipitation of calcium salts can result in deterioration of kidney function. Of note, in recent years
the incidence of hypercalcemia in newly diagnosed
patients has dropped to 10%–15%, most likely
because of earlier diagnosis. In Latin America and
some parts of Asia where late diagnosis is common,
hypercalcemia remains more common.
Hyperviscosity resulting from high myeloma protein levels can cause problems such as bruising, nose
bleeding, hazy vision, headaches, gastrointestinal
14
bleeding, sleepiness, and a variety of ischemic neurological symptoms caused by reduced blood and
oxygen supply to the nerve tissue. Hyperviscosity
occurs in < 10% of patients with myeloma and in
about 50% of patients with Waldenström’s macroglobulinemia (all of whom have IgM paraprotein or
M-component). Increased bleeding is often exacerbated by thrombocytopenia as well as by binding
of monoclonal proteins to clotting factors and/or
platelets.
Neurologic involvement can result in specific problems depending on the location of affected nerves.
Particularly common problems are spinal cord compression, meningitis, and carpal tunnel syndrome.
Although the first two are due to plasma cell tumor
formation or infiltration, carpal tunnel syndrome is
usually due to amyloid deposition (deposition of
Bence Jones proteins in a special beta-pleated form).
Staging and prognostic factors
Prognosis in myeloma is determined by both the
number and specific properties of myeloma cells
in a given patient. These specific properties include
the growth rate of myeloma cells, the production
rate of monoclonal proteins, and the production or non-production of various cytokines and
chemicals that damage or significantly impair
other tissues, organs, or bodily functions. In 1975,
the Durie-Salmon Staging System was developed
(see Table 4). This system brings together the major
clinical parameters in correlation with measured
myeloma cell mass (the total number of myeloma
cells in the body). The Durie-Salmon Staging System continues to be used worldwide, primarily
because it provides the best direct correlation
with individual patient clinical features. Stage I
patients have smoldering disease; Stage II and III
patients have active myeloma. In 2005, a new staging system was developed by the IMF-sponsored
IMWG. Clinical and laboratory data were gathered
on 10,750 previously untreated symptomatic
myeloma patients from 17 institutions, including
sites in North America, Europe, and Asia. Potential
prognostic factors were evaluated using a variety
of statistical techniques. Serum β2 microglobulin
(Sβ2M), serum albumin, platelet count, serum creatinine, and age emerged as powerful predictors of
survival and were then further analyzed.
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Table 4. Durie-Salmon Staging System
STAGE
CRITERIA
MEASURED MYELOMA CELL MASS
(myeloma cells in billions/m2)*
STAGE I
(low cell mass)
All of the following:
• Hemoglobin value > 10 g/dL
• Serum calcium value normal or < 10.5 mg/dL
• Bone x-ray, normal bone structure (scale 0),
or solitary bone plasmacytoma only
• Low M-component production rates
IgG value < 5 g/dL;
IgA value < 3 g/dL
Urine light chain M-component on electrophoresis < 4 g/24h
600 billion*
STAGE II
(intermediate cell mass)
Fitting neither Stage I nor Stage III
600 to 1,200 billion*
STAGE III
(high cell mass)
One or more of the following:
• Hemoglobin value < 8.5 g/dL
• Serum calcium value > 12 mg/dL
• Advanced lytic bone lesions (scale 3)
• High M-component production rates
IgG value > 7 g/dL;
IgA value > 5 g/dL
Urine light chain M-component on electrophoresis > 12 g/24h
> 1,200 billion*
SUBCLASSIFICATION
(either A or B)
• A: relatively normal renal function (serum creatinine value) < 2.0 mg/dL
• B: abnormal renal function (serum creatinine value) > 2.0 mg/dL
Examples: Stage IA (low cell mass with normal renal function);
Stage IIIB (high cell mass with abnormal renal function)
*myeloma cells in the whole body
A combination of serum β2 microglobulin and
serum albumin provided the most, powerful, simple, and reproducible three-stage classification.
The ISS was fully validated and is shown in Table 5.
The ISS was further validated by demonstrating
effectiveness in patients in North America, Europe,
and Asia; in patients younger and older than age
65 years; with standard therapy or auto transplant;
and in comparison with the Durie-Salmon Staging
System. The ISS is simple, based upon easy-to-use
variables (serum β2M and serum albumin), and has
been introduced for widespread use.
Myeloma can be further classified based upon
genetic risk using molecular fluorescence in situ
hybridization (FISH) and cytogenetic features
identified in bone marrow myeloma cells. Such
classification can have important implications for
treatment. Higher-risk disease is defined as the presence of any one of the following genetic mutations:
t(4;14), t(14;16), t(14;20), deletion of 17p by FISH, or
myeloma.org
deletion of chromosome 13 or hypodiploidy by conventional metaphase cytogenetics. It is crucial to be
aware that treatment selection is very much influenced by genetic risk. For example, the presence of
t(4;14), which has been noted as a poor risk factor
in the past, has largely been overcome with the
introduction of Velcade (bortezomib) combination
Table 5. International Staging System (ISS)
STAGE
VALUES
STAGE 1
β2M < 3.5 mg/L
ALB ≥ 3.5 g/dL
STAGE 2
β2M < 3.5 mg/L
ALB < 3.5 g/dL
or
β2M = 3.5–5.5 mg/L
STAGE 3
β2M > 5.5 mg/L
β2M = Serum β2 microglobulin, ALB = Serum albumin
15
regimens. There is also a positive impact of lenalidomide-containing regimens in patients with t(4;14)
in several Revlimid trials. A recent report from the
IFM group indicated that the presence of t(14;16)
was also no longer a predictive prognostic factor in
their trials, while IFM findings published in February 2015 indicate that in early relapse, Pomalyst is
an effective treatment for those with deletion 17p.
New and better risk classification systems are being
developed and evaluated with the expectation that
it will be possible to offer treatment selection based
upon documented treatment outcomes with new
combination approaches.
One such new risk classification system is microarray-based gene expression profiling (GEP), which
has been used to assess risk in myeloma patients
both at diagnosis and at relapse. Approximately
15% of newly diagnosed patients assessed with
GEP in clinical trials have shown a high-risk GEP
signature. Such patients have shorter durations of
complete remission, event-free survival, and OS.
While GEP has the potential to further refine risk
prognosis beyond standard cytogenetics (karyotyping) and FISH, its use is currently limited by the
lack of a uniform platform across many centers in
the world and by widespread unavailability.
Table 6. IMWG Uniform Response Criteria – CR and Other Response Categories
RESPONSE
SUBCATEGORY
RESPONSE CRITERIAa
sCR
CR as defined below plus
• Normal FLC ratio, and
• Absence of clonal cells in bone marrowb by immunohistochemistry or immunofluorescencec
CR
• Negative immunofixation on the serum and urine, and
• Disappearance of any soft-tissue plasmacytomas, and
• ≤ 5% plasma cells in bone marrowb
VGPR
• Serum and urine M-protein detectable by immunofixation but not on electrophoresis, or
• 90% or greater reduction in serum M-protein plus urine M-protein level < 100 mg per 24h
PR
• ≥ 50% reduction of serum M-protein and reduction in 24h urinary M-protein by ≥ 90% or to < 200 mg per 24h
• If the serum and urine M-protein are unmeasurable, a ≥ 50% decrease in the difference between involved and
uninvolved FLC levels is required in place of the M-protein criteria
• If serum and urine M-protein are unmeasurable, and serum free light chain assay is also unmeasurable,
≥ 50% reduction in plasma cells is required in place of M-protein, provided baseline bone marrow plasma
percentage was ≥ 30%
In addition to the above listed criteria, if present at baseline, a ≥ 50% reduction in the size of soft tissue
plasmacytomas is also required
SD
Not meeting criteria for CR, VGPR, PR, or progressive disease (not recommended for use as an indicator of response,
stability of disease is best described by providing the time to progression estimates)
Abbreviations: CR = complete response; FLC = free light chain; PR = partial response; SD = stable disease;
sCR = stringent complete response; VGPR = very good partial response.
a – All response categories require two consecutive assessments made at anytime before the institution of any new therapy;
all categories also require no known evidence of progressive or new bone lesions if radiographic studies were performed.
Radiographic studies are not required to satisfy these response requirements.
b – Confirmation with repeat bone marrow biopsy not needed.
c – Presence/absence of clonal cells is based upon the κ/λ ratio. An abnormal κ/λ ratio by immunohistochemistry and/or
immunofluorescence requires a minimum of 100 plasma cells for analysis. An abnormal ratio reflecting presence of an abnormal
clone is a κ/λ ratio of > 4:1 or < 1:2.
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Definition of clinical response
The IMWG uniform response criteria are recommended to classify response (see Table 6). Improvements in M-component must be associated with
evidence of clinical improvement (such as reduced
bone pain and/or improved red blood cell counts).
It is important to keep in mind that a higher percent
regression does not automatically confer longer
survival. When there is residual disease, the characteristics of the remaining drug-resistant myeloma
cells determine the outcome. These remaining
myeloma cells may, or often may not, have any tendency for immediate regrowth (relapse). If there is
no regrowth, this is what is called “plateau phase”:
residual, but stable disease. The fraction of resistant myeloma cells is primarily dependent upon
the intrinsic molecular features of the individual
myeloma and the pre-treatment tumor burden or
stage. Responding patients go from a high-risk to a
lower-risk status until, ideally, no signs of myeloma
are left, or they reach a stable plateau phase, but
with measurable residual disease. The time required
to reach the plateau phase is variable, ranging from
3 to 6 months (rapid response), to 12 to 18 months
(slow response). (See Figure 4.)
As treatments have improved, it has become more
important to assess response to treatment as accurately as possible. Besides the depth of response,
which is indicated by PR (≥ 50% improvement),
VGPR (≥ 90%), or CR (100% reduction in monoclonal protein) (see Table 6), one must now consider even deeper responses as well as duration
of response. With the increasing efficacy of new
combination therapies, it is now necessary to add
the terms “minimal residual disease (MRD)” and
“MRD-negative” to the response criteria, concepts
that were previously unattainable and unmeasurable in myeloma. Minimal disease levels are now
not only possible to achieve, but are verifiable with
next-generation sequencing and next-generation
flow, a highly sensitive and specific new type of flow
cytometry performed on bone marrow that was
developed at the University of Salamanca, Spain.
The FDA has endorsed this new 8-color flow test as
the standard means to measure depth of response
in US-based myeloma clinical trials. In addition,
another sensitive new test, the heavy/light chain
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assay, will be incorporated into response criteria
as a blood marker of low-level disease activity.
New IMWG response criteria defining MRD and the
tests used to verify it are in process at the time of
this writing.
Important terms are:
— T TP – Time To Progression: the time from start of
treatment until relapse occurs.
— PFS – Progression-Free Survival: the length of survival during which the patient is still in remission*.
FS1 – As defined by Palumbo, the time from
¡P
the start of therapy to the occurrence of first
relapse.
FS2 – The time from start of therapy to the
¡P
occurrence of second relapse, incorporating the duration of both first and second
remissions.
*Remission is generally considered to be at least a
partial response (PR, ≥ 50% improvement) which
lasts for at least 6 months.
Treatment
Exclude MGUS or asymptomatic myeloma
The first and most important decision is to determine if treatment is required. Patients with
MGUS and asymptomatic or smoldering multiple
myeloma (see Table 1) should be observed closely
rather than treated. There are currently several
clinical trials that are attempting to determine if it
is possible to enhance the immune regulation of
early myeloma or reduce the likelihood of disease
activation.
Of note are two completed studies: the Spanish
group’s (PETHEMA) trial for high-risk SMM in which
patients were either observed or treated with lenalidomide and dexamethasone, and the NCI study of
carfilzomib, lenalidomide, and dexamethasone for
patients with high-risk SMM. In the Spanish trial, disease progression was delayed and OS at 3 years was
significantly improved among patients who were
treated with lenalidomide and low-dose dexamethasone as compared to those who were observed.
In the NCI pilot study, which was presented at ASH
2014, the combination of carfilzomib, lenalidomide,
and dexamethasone in the 12 enrolled patients
resulted in a 100% complete response rate over the
17
course of the study. Moreover, 11 of the 12 patients
who responded were MRD negative. They are currently being followed to assess the duration of their
MRD-negative status.
A large, ongoing, combined ECOG/SWOG trial
was started in 2010, in which patients with highrisk SMM are randomized to lenalidomide versus
placebo. Many other trials are now available for
patients with high-risk SMM, some of which incorporate experimental agents. There is as yet, however, no universally accepted definition of what
constitutes high-risk SMM. The criteria for high-risk
SMM vary from trial to trial, making it difficult to
standardize a definition.
The IMWG has recently published Updated Criteria
for the Diagnosis of Myeloma (Rajkumar SV et al.,
The Lancet) in order to accurately identify “the subset of patients with smoldering multiple myeloma
and biological malignancy who are at imminent
risk of developing CRAB features.” The validated criteria for “ultra-high-risk” SMM are defined as:
— at least 60% plasmacellularity of bone marrow;
— a ratio of involved to uninvolved free light chains
of at least 100;
— 2 or more focal lesions on MRI.
Because these criteria have individually been
proven to carry an 80% or greater risk of progression to active disease within 18 months to 2 years,
any one of them is considered a “myeloma-defining event.” Thus, asymptomatic patients with any of
these criteria should be considered to have early
active myeloma and should be treated, not merely
observed. This is a major paradigm shift in myeloma,
as previous wisdom held that all asymptomatic
patients be observed until one or more of the CRAB
criteria were manifest. Because there are now treatment tools available to prevent disease progression
and potentially to cure myeloma before it causes
end-organ damage, it is now imperative to intervene in cases of early active disease.
Specific anti-myeloma treatment is recommended
when active myeloma has developed, as reflected
by an increasing M-component and/or emerging or imminent clinical problems or “CRAB” features (See Table 1). Problems sufficient to require
treatment include bone destruction (lytic lesions
18
and/or osteoporosis), renal insufficiency, progressive reduction in blood counts (e.g., anemia, neutropenia), elevated blood calcium, nerve damage,
or other significant organ or tissue damage caused
by myeloma or myeloma protein. These indications
for the need to start treatment can be summarized
as CRAB features: Calcium elevation; Renal problems; Anemia; or Bone issues. The overall goals of
treatment are to address specific problems and to
achieve general control of the disease. A summary
of types of treatments is provided in Table 7.
Treatment overview
Please see the History section for an overview of the
evolution of currently used treatments. Since melphalan was first introduced in 1962, various combination chemotherapy regimens have been utilized
and attempts have been made to improve outcomes using high-dose chemotherapy regimens
with bone marrow transplant (BMT) or peripheral
blood stem cell transplant (PBSCT). In the standard
type of BMT or PBSCT, the “transplant” is a “rescue”
with normal bone marrow stem cells after the stem
cells in the body have been destroyed by high-dose
chemotherapy (usually melphalan).
In the 1980s and 1990s, high-dose melphalan with
stem cell rescue was one of the few techniques
available to reduce myeloma tumor burden and
achieve better outcomes. With the introduction
of thalidomide for myeloma treatment in 1997,
the options for treatment expanded. Complete
responses could be achieved with a simple oral
agent. Additional novel agents followed in rapid
succession: first Velcade (bortezomib, 2003), then
Revlimid (lenalidomide, 2005), Kyprolis (carfilzomib,
2012), Pomalyst (pomalidomide, 2013), and most
recently, Farydak (panobinostat, 2015). Experimental agents with novel mechanisms of action such as
elotuzumab, selinexor, and the anti-CD 38 monoclonal antibodies daratumumab and SAR650984
are showing promising results, as are the oral
proteasome inhibitors. It has become increasingly
clear that no single therapy is likely to be effective
for every myeloma patient, nor is any single agent
likely to achieve a cure on its own. Rather, the combination approach that attacks myeloma cells with
multiple drugs through multiple pathways has thus
far demonstrated superior efficacy.
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There is no simple answer to the question of “the
best” treatment options available in 2015. Fortunately, there are numerous regimens that produce
very deep responses, durable responses (remissions lasting ≥ 2 years), and improved OS. The best
choice for each patient depends upon individual
factors such as age, stage, genetic features, kidney status, comorbidities, and of course, personal
preference.
Myeloma patients must be aware of the need for
careful discussions with their physicians about
treatment choices.
Table 7. Myeloma Treatment Options
1. Induction Therapy
2. High-dose chemotherapy with hematopoietic stem
cell transplant
3. Conservative use of radiation to preserve bone marrow
4. Maintenance therapy
5. Supportive care:
• Pain medication
• Anti-viral therapy
• Bisphosphonates
• Brace/corset
• Growth factors
• Kyphoplasy/vertebroplasty
• Antibiotics
• Exercise
• Emergency care
(e.g., dialysis, plasmapheresis, surgery, radiation)
6. Management of drug-resistant or refractory disease
7. New and emerging treatments:
• Immunomodulatory drugs (IMiDs)
Thalomid® (thalidomide), Revlimid® (lenalidomide),
Pomalyst® (pomalidomide)
• Approved IV proteasome inhibitors
Velcade® (bortezomib) and Kyprolis® (carfilzomib),
and experimental oral proteasome inhibitors
oprozomib, ixazomib, and marizomib in clinical trials
• Histone deacetylase (HDAC) inhibitor
Farydak® (panobinostat); HDAC inhibitor
rocilinostat (ACY-1215) in clinical trials
• Anti-SLAMF7 monoclonal antibody elotuzumab in
late-phase studies in combination with lenalidomide
and dexamethasone and in combination with other
approved and experimental agents
• Anti-CD38 monoclonal antibodies daratumumab
and SAR650984 in clinical trials
• Pan-tumor suppressor gene promoter selinexor
in clinical trials
myeloma.org
Options for patients who
are not candidates for
stem cell transplant
The approach to frontline treatment has changed
substantially with the introduction of the novel
agents thalidomide, bortezomib, lenalidomide,
and carfilzomib. Selection of frontline therapy
should be tailored to the patient’s fitness status
and to the presence or absence of kidney disease,
peripheral neuropathy, and high-risk genetic mutations. At the present time, 98% of patients in the
US receive induction therapy that includes at least
one novel agent. A recent registry survey showed
that Revlimid/dexamethasone and Velcade-based
combinations are used in approximately equal
numbers in the frontline setting, with thalidomide/
dexamethasone now less frequently used, primarily because of the availability of next-generation
IMiDs and their relatively favorable side effects
profile in contrast to thalidomide-related adverse
events that include thrombosis, fatigue, cytopenia,
and peripheral neuropathy.
The 2015 NCCN Guidelines for treatment of
patients who are not candidates for high-dose
therapy with stem cell transplant include Velcade/
dexamethasone (VD) at category 2A, and, in category 1, Revlimid/low-dose dexamethasone (Rd);
melphalan/prednisone/Velcade (MPV); melphalan/
prednisone/Revlimid (MPR); and melphalan/prednisone/thalidomide (MPT). The 2013 publication
of the IFM’s three-arm FIRST trial comparing continuous Revlimid/dexamethasone therapy to fixeddose Revlimid/dexamethasone and to melphalan/
prednisone/thalidomide has, however, not only
demonstrated the superiority of continuous therapy with lenalidomide over fixed-dose Revlimid or
MPT, but has also called into question the use of
melphalan combinations in the frontline treatment
of newly diagnosed patients who are not eligible
for stem cell transplant.
The International Myeloma Working Group consensus statement for the management, treatment, and
supportive care of patients with myeloma not eligible
for standard autologous stem cell transplantation
(Palumbo A. et al. JCO January 13, 2014) recom­
mends that these older and sometimes frailer
patients be treated according to their fitness level. To
this end, Dr. Antonio Palumbo and his team in Torino,
19
Italy, developed a geriatric assessment tool (Palumbo
A. et al. Geriatric assessment predicts survival and toxicities in elderly myeloma: an International Myeloma
Working Group report. Blood January 27, 2015) to
assess comorbidities and cognitive and physical status. The tool predicts mortality and the risk of toxicity in elderly myeloma patients, the better to tailor
therapy appropriately. The guidelines recommend
that while it is usually preferable to treat the elderly
frail patient with a two-drug regimen (Velcade/
dexamethasone or Revlimid/dexamethasone), fit,
newly diagnosed patients who are not eligible for
transplant should be treated with three-drug regimens such as RVD or its variant, reduced-dose “VRD
lite”; CyBorD (cyclophosphamide/bortezomib/dexamethasone); and more commonly outside the US,
CTD (cyclophosphamide/thalidomide/dexamethasone) or VMP (Velcade/melphalan/prednisone). (See
Table 8.)
At the 2014 ASH meeting, Dr. Maria-Victoria
Mateos from the Salamanca group presented data
demonstrating that for non-transplant-eligible
patients, VMP and Rd can be given either sequentially or alternatively, with equivalent outcomes for
either approach.
If stem cell harvest is planned
A basic caveat for transplant-eligible patients is
the avoidance of melphalan-containing induction regimens, since melphalan can damage
bone marrow. Older age (> 70 years) is not an
absolute deterrent to stem cell transplant. Whether
Table 8. Frontline Treatment Options
for Patients Not Eligible for Transplant
Frail Patients: Two-drug Regimen
• Revlimid + low-dose dexamethasone (Rd)
• Velcade + low-dose dexamethasone (Vd)
Fit Patients: Three-drug Regimen
• Velcade/Revlimid/dexamethasone (VRD or RVD)
• Reduced-dose VRD (VRD-lite)
• Velcade/Cytoxan/dexamethasone (VCD or CyBorD)
• Velcade/thalidomide/dexamethasone (VTD)
• Cytoxan/thalidomide/dexamethasone (CTD)
• Velcade/melphalan/prednisone (VMP)
• VMP ± Rd (sequential or alternating)
• Other
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or not autologous transplant is an appropriate
option must be discussed with each patient on an
individual basis, taking into account fitness, genetic
risk factors, family and work considerations, and
personal preference.
It has become an open question whether auto
transplant as a part of first-line treatment is required
or whether it can be offered as an option at first
relapse or later. We await the results of three definitive Phase III clinical trials in 2015 and 2016 that
will answer this question. Recently, the data from
a Phase II IFM study of VRD induction followed by
upfront high-dose therapy with autologous stem
cell transplant, VRD consolidation, and one year
of Revlimid maintenance demonstrated a further
20% increase in depth of response after transplant
beyond that achieved with induction VRD (Roussel
M et al. JCO July 2014). Given this and other data
on upfront transplant, it is reasonable to proceed
with the transplant as part of frontline therapy for
transplant-eligible patients while awaiting Phase III
trial results.
The approach to frontline or induction therapy prior
to stem cell harvest and high-dose therapy with
stem cell rescue has evolved and changed considerably over the last two decades. The former standard
induction regimen has now been supplanted by more
effective combination regimens with less toxicity.
The NCCN category 1 recommendations for primary
therapy of transplant candidates include Velcade/
dexamethasone (VD); Velcade/doxorubicin/dexamethasone (PAD); Velcade/thalidomide/dexamethasone (VTD); and Revlimid/dexamethasone (Rd). Stem
cell harvesting following Revlimid/dexamethasone
may require a growth factor plus cyclophosphamide
or plerixafor, as opposed to growth factor alone (e.g.,
Neupogen®). Cyclophosphamide/bortezomib/dexamethasone (CyBorD); Velcade/Revlimid/dexamethasone; and carfilzomib/Revlimid/dexamethasone
(CRD) are all ranked at category 2A, and several other
combination therapies are listed as category 2B: dexamethasone monotherapy; Doxil/vincristine/dexamethasone (DVD); and thalidomide/dexamethasone
(TD). The consensus in 2015 is that three-drug combination therapies are recommended as induction prior
to ASCT.
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Caveats for various induction options
Three-drug regimens can produce rapid responses
and have high response rates. Regimens containing
Revlimid and dexamethasone carry an increased
risk of blood clots (deep vein thrombosis, or DVT)
and require prophylactic aspirin or other anticoagulant treatment. Neuropathy is a concern with the
thalidomide- and Velcade-containing regimens.
Supplements such as the amino acids L-carnitine
and L-glutamine and vitamins B6 and B12 may
offer some neuroprotection. A new mRNA test is in
development that would identify myeloma patients
at risk for bortezomib-induced peripheral neuropathy, thus guiding treatment selection ahead of time.
The incidence of peripheral neuropathy has been
demonstrated to be significantly less with subcutaneous Velcade than with IV administration. Velcade
increases susceptibility to herpes zoster infection
(shingles). Patients taking Velcade should therefore
be given antiviral therapy prophylactically.
The Phase II IFM study referenced above in which
patients were given VRD induction, ASCT, VRD consolidation, and one year of Revlimid maintenance
may point the way to a new standard of care among
transplant-eligible patients in the future. 68% of
the patients were MRD-negative by flow cytometry
after completion of the study. With 39 months of
follow-up at study publication, overall survival was
100%, and none of those who were MRD-negative
had relapsed. These data are a preview of the ongoing IFM/Dana-Farber Phase III study whose final
results we await later in 2015 or 2016.
It is a challenge to select the best treatment for
each patient. One must consider the early risks
of treatment, responses and length of remission,
DVT and neuropathy risks, convenience, and costs.
Presence of genetic high-risk features and/or renal
compromise may sway the choice toward Velcade
combinations. Open dialogue to discuss the “pros
and cons” is crucial.
Transplantation
High-dose therapy (HDT) with autologous
stem cell transplantation (ASCT)
— The role of autologous transplantation has been
extensively reviewed, and remains a topic under
investigation in both the upfront and relapse, or
salvage, settings.
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Table 9. Induction Therapy Options
for Transplant-Eligible Patients
Velcade-based triple therapy
• VCD (CyBorD) (Velcade, Cytoxan, dexamethasone)
• VRD (RVD) (Velcade, Revlimid, dexamethasone)
• VTD (Velcade, thalidomide, dexamethasone)
• PAD (Velcade, Adriamycin, dexamethasone)
Kyprolis-based triple therapy
• KCD (Kyprolis, Cytoxan, dexamethasone)
• KRD (Kyprolis, Revlimid, dexamethasone)
• KTD (Kyprolis, thalidomide, dexamethasone)
• Other
— HDT with autologous stem cell transplantation
has been shown to improve both response rates
and survival in patients with myeloma. However,
this approach is not curative. With the introduction of novel combination therapies in addition
to ASCT, some investigators are introducing the
notion that a subgroup of patients (“good risk”)
may have extended survival and may achieve
“functional cure” (defined as complete remission
for ≥ 4 years).
— Complete remission rates with HDT as a planned
part of frontline therapy can now be ≥ 90% with
new pre- and post-transplant strategies, with PFS
rates extending to four years.
— The added benefit of incorporating autotransplantation or not, and whether it is best to do it
upfront or delay transplant until relapse is under
ongoing review, with the results of three definitive clinical trials expected within the next year.
— Morbidity and mortality – With current growth
factor, antibiotic, and other supportive care, the
procedure-related mortality with HDT is very low:
< 5%. The majority of centers use intravenous
high-dose melphalan alone at a dose of 200 mg/m2
as the preparative regimen.
Current Recommendations
HDT with autologous stem cell support should
be recommended as part of the frontline therapy for eligible newly diagnosed patients with
symptomatic myeloma.
a.The standard conditioning regimen is melphalan 200 mg/m2. Total body irradiation is not
recommended.
21
b. Stem cell purging is not recommended because
of added expense without additional clinical
benefit.
c. Peripheral blood stem cells are recommended
over bone marrow because of ease of collection
and more rapid engraftment.
d. The pre-transplant regimens are discussed above.
Role of auto transplantation
at time of first relapse
Part of the decision process for autotransplant
involves knowledge of the impact of waiting, with a
view to transplant at relapse. Data from two French
randomized trials and a Mayo Clinic retrospective
study indicate no reduction in overall survival from
waiting to do the transplant at relapse. Neither of
these studies, however, examined the impact of
induction therapy with the powerful combination
of a combined IMiD and proteasome inhibitor. The
large, randomized US-French trial of frontline VRD
versus VRD + ASCT, mentioned above with results
still pending, will help to determine if the addition
of consolidation with ASCT after best novel therapy
provides additional benefit or not. Quality of life
becomes an important consideration. On the one
hand, if transplant is not performed as a planned
primary strategy, then typically additional therapy, including maintenance, is required, with corresponding toxicity and side effects. On the other
hand, the major impact of the transplant is deferred,
which for some patients is a better personal choice.
Table 10. Most Commonly Used Chemotherapy Drugs
DRUG NAME
OTHER TREATMENT NAME
COMMENTS
melphalan*
(M)**
Alkeran®
(by mouth or IV)
Best single agent for treatment
cyclophosphamide*
(C or CY)**
Cytoxan®
(by mouth or IV)
Bis-chloro-Nitrosourea®
Similar efficacy to M but with more GI and GU toxicity and less bone
marrow stem cell injury
prednisone
(P)**
Prednisolone® (similar)
(usually by mouth)
Directly active, works well with M, C, and B.
Does not produce suppression of bone marrow
dexamethasone
(D)**
Decadron®
(by mouth or IV)
Similar to prednisone but more potent; more severe side effects
Pegylated, liposomal
doxorubicin*
Doxil®
(IV)
In combination, promising activity, less toxicity than A
bortezomib
(B, V, or P)**
VELCADE®
(IV)
Directly active, used alone or in combination
thalidomide
(T)**
Thalomid®
(by mouth)
Directly active, approved for use in combination with dexamethasone,
used in other combinations
lenalidomide
(R or L)**
Revlimid®
(by mouth)
Directly active, approved for use in combination with dexamethasone,
used in other combinations
carfilzomib
Kyprolis® (IV)
Directly active, used alone or in combination
pomalidomide
Pomalyst® (by mouth)
Directly active, used alone or in combination
panobinostat
Farydak® (by mouth)
Approved for use in combination with bortezomib and dexamethasone
Traditional Agents
Novel Agents
*Alkylating agents **Common abbreviation
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Harvesting and storing stem cells
for later use
There is a strong reluctance in many centers to harvest stem cells without a clear plan for use, typically
immediate use. This reluctance arises from protocol
priorities, cost/utilization constraints for harvesting
and storage, as well as numerous other factors.
Nonetheless, many patients request and want their
stem cells harvested, even though they may not be
enthusiastic about immediate high-dose therapy.
Current Recommendations
a. Harvesting with storage for future use is recommended with review on a case-by-case basis.
b. There is medical and scientific rationale for saving stem cells for later use.
c. Delayed transplant is a viable treatment option.
d. A second transplant at relapse is a viable option,
especially if a first remission following transplant of > 2 years has occurred. (See discussion of
“double” transplantation.)
The role of double or
tandem transplantation
— At present the added benefit of double or tandem transplantation versus a single autologous
transplant is unclear.
— The results with planned primary tandem transplant (Total Therapy 1, 2, 3, 4, and 5 at the University of Arkansas) have been good. The median
overall survival has been 68 months, with some
sub-groups having even longer survival. Total
Therapy 3, which incorporates the use of Velcade,
appears to offer earlier response and increased
response rates, although patients with high-risk
factors, including older age, higher LDH, abnormal cytogenetics, or advanced disease, are not as
likely to achieve extended benefit.
— Comparative studies, including the French randomized studies, have shown benefit predominantly for a subgroup of patients (those who are
not in VGPR or CR).
Current Recommendations
a. At the present time, planned tandem transplant
continues to be a clinical trial option and should
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be carried out at centers specialized in this
approach. A planned second transplant can be
considered in patients achieving < VGPR with a
first auto transplant.
b.A second transplant in a patient who has
responded well with a first transplant and relapsed
after > 2 years is a helpful and viable option.
c. Saving and storing enough stem cells for a second or additional transplant, if appropriate, is
strongly recommended.
The role of allogeneic transplantation
— Despite medical improvements over the past two
decades, full allogeneic transplant, even with
a perfectly matched sibling donor, is a high-risk
procedure in the management of myeloma. The
initial treatment-related morbidity and mortality
is high. Even at centers with the greatest experience, and in the best risk settings, initial mortality
is at least 15% to 20%. In other centers, 20% to
30% or higher mortality is frequently reported.
The pulmonary complications are usually the
most critical for patients with myeloma.
— The potential advantages of allogeneic transplantation are myeloma-free stem cells and graft-versus-myeloma effect. But, despite these factors,
long-term cure is rare. Relapse continues at a rate
of approximately 7% per year with long-term
follow-up. Graft-versus-host disease (GVHD) can
also be an ongoing problem, requiring therapy
and reducing quality of life.
— The graft-versus-myeloma effect can be enhanced
by using donor lymphocyte infusions and has
been clinically beneficial in some series.
— A cooperative group trial evaluating 710 patients
randomized to non-myeloablative or “mini”
allogeneic transplant versus tandem autologous
transplant was presented at ASH 2010 (Krishnan
et al.). Unfortunately, this trial showed rather decisively that planned addition of mini-allo transplant
as part of an upfront double-transplant approach
introduced significant added risk with no survival benefit over tandem autologous transplant.
Thus, routine consideration of this approach is no
longer recommended.
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Current Recommendations
a. Conventional full-match allogeneic transplantation is rarely recommended as a primary strategy because the risks are too high.
b. “Mini” allogeneic transplantation is only recommended in a clinical trial setting. There has been
increasing interest in the upfront use of allogeneic transplant for high-risk patients.
c. Identical twin, or “syngeneic” transplantation is a
rare option, which is a safe procedure with good
outcome and is recommended as a consideration when an identical twin is available.
Radiation
Radiation therapy is an important
modality of treatment for myeloma.
For patients with severe local problems such as bone
destruction, severe pain, and/or pressure on nerves
or the spinal cord, local radiation can be dramatically
effective. The major disadvantage is that radiation
therapy permanently damages normal bone marrow stem cells in the area of treatment. Wide-field
radiation encompassing large amounts of normal
bone marrow should be avoided. A general strategy
is to rely on systemic chemotherapy to achieve overall disease control, limiting the use of local radiation
therapy to areas with particular problems.
Table 11. High-Dose Therapy
TRANSPLANT TYPE
ADVANTAGES
DISADVANTAGES
Single Autologous
• 50% excellent remissions
• At least as good as standard therapy regarding
overall survival and probably better for patients
with high Sβ2M
• Basis for strategies to produce true remission or
long-term cure
• New preparative regimens may produce true
complete remission
• Relapse pattern similar to standard chemotherapy
• More toxic and expensive
• Patients who decisively benefit from transplant
not clearly identified
• Maintenance therapy may still be
required/ recommended
Double Autologous
• 2002 update of French data indicates survival
benefit for subset of patients not in CR or VGPR
• Excellent results with tandem transplant
(see text)
• Role of double versus single still unclear
• Much more toxic and expensive versus single
• No survival benefit if in CR or VGPR after
first transplant
Traditional Allogeneic
• No risk of contamination of marrow/stem cells
with myeloma
• Possible graft-versus-myeloma effect to
prolong remission
• Even for HLA identical siblings, significant risk of
early complications and even death (25%–30%)
• Risk of complications unpredictable
• Restricted to age < 55
• More toxic and expensive versus autologous
Mini-Allo
• Less toxic form of allo
• Preparative chemotherapy usually well tolerated
• Results in anti-myeloma immune graft
• No anti-myeloma chemotherapy given
• Still produces graft-versus-host disease
• Full benefits still unclear
• Risk of initial mortality approximately 17%
• Not recommended for myeloma patients outside
the context of a clinical trial
Identical Twin
• No risk of myeloma contamination in
transplanted cells
• Much less risky than allogeneic transplant
• No graft-versus-myeloma effect
• Need identical twin < 55
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Maintenance therapy
Immunomodulatory drugs (IMiDs)­– In 2012,
three randomized placebo-controlled trials
reported a significant prolongation of progression-free survival with Revlimid as maintenance
therapy for myeloma. Two of these trials looked
at post-transplant maintenance, and the third
trial evaluated Revlimid as maintenance following
standard melphalan-based therapy. The US CALGB
study (McCarthy et al.) concluded that Revlimid at a
dose of 10 mg per day for 21 out of 28 days doubles
time to progression compared with placebo when
given to patients with stable disease or better
after high-dose melphalan/ASCT. Follow-up data
from that trial demonstrated that Revlimid maintenance also increases overall survival. The IFM
study demonstrated that Revlimid maintenance
significantly prolongs progression-free survival
when given to patients after ASCT as consolidation
therapy followed by a lower dose of Revlimid for
maintenance therapy, but has no impact on overall
survival (Attal et al.).
Balanced against the favorable data on maintenance with Revlimid is the low but increased
risk of a second malignancy. A follow-up study
by Palumbo of the Italian group determined that
Revlimid alone does not increase the risk of second
malignancy, but that the combination of melphalan
and Revlimid, two agents that can take a toll on the
bone marrow, does. We await the results of longterm follow-up with the Revlimid maintenance trials as well as results of several maintenance trials
with approved and experimental agents.
Velcade – A HOVON/GMMG Phase III study comparing Velcade, Adriamycin, and dexamethasone
(PAD) + Velcade maintenance, to vincristine, Adriamycin, and dexamethasone (VAD) + thalidomide
maintenance, was published in August 2012. Not
only did Velcade result in improved PFS and OS, but
its use as maintenance therapy administered on an
every-other-week schedule was well tolerated and
resulted in additional responses. Initial results also
indicated benefit in patients with the deletion 17p
poor-risk FISH genetic feature.
Supportive care
Bisphosphonates – Bisphosphonates are a class
of chemicals that bind to the surface of damaged
bones in patients with myeloma. This binding
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inhibits ongoing bone destruction and can improve
the chances of bone healing and recovery of bone
density and strength. A randomized study utilizing
the bisphosphonate pamidronate (Aredia) showed
particular benefit in patients responding to ongoing chemotherapy (see Figure 5). The IMWG’s 2013
recommendations for the treatment of myeloma-related bone disease state that bisphosphonate therapy should be considered in all patients
receiving first-line anti-myeloma therapy, regardless of the presence of osteolytic bone lesions on
conventional radiography. Other bisphosphonates
available include clodronate (Bonefos®), an oral
formulation in use in Europe for the treatment
of myeloma bone disease, and zoledronic acid
(Zometa), approved in the US and Europe as treatment of both hypercalcemia and bone disease.
Several new therapies to prevent myeloma-related
bone loss are in clinical trials, including denosumab,
a monoclonal antibody to RANK ligand, BHQ880, an
anti-DKK1 monoclonal antibody, and sotatercept, a
fusion protein that stimulates bone growth.
Figure 5. How Pamidronate Works
At the 2010 annual meeting of the American Society of Hematology, a randomized comparison of
zoledronic acid with clodronate as part of the MRC
Myeloma IX trial (Morgan et al.) showed that zoledronic acid was not only superior to clodronate in
preventing skeletal-related events (SRE), but also
provided a survival benefit independent of SRE
reduction, supporting anti-myeloma activity of
zoledronic acid.
Several concerns have emerged related to chronic
bisphosphonate use. Two of these, kidney damage
and ONJ are addressed in detail in other IMF educational materials (Myeloma Minute, Myeloma Today,
and Understanding Bisphosphonate Therapy). Both
conditions are fortunately relatively uncommon,
but awareness of these potential problems is the
25
key to prevention. Kidney function must be serially
monitored (especially serum creatinine before each
treatment dose), particularly with Zometa use. If
the serum creatinine increases by 0.5 to 1.0 mg/dL,
dose and/or schedule adjustments for Aredia or
Zometa may be required. For Zometa, one of the
simplest adjustments is to extend the infusion time
from 15 minutes to 30–45 minutes, which reduces
the risk of renal impairment.
recommended. Any major jaw surgery must be
avoided until consultation has been sought.
Dental extractions should be avoided until full
consultation has been obtained as well. Infection
may require antibiotic therapy. In recent years the
incidence of ONJ appears to have decreased dramatically in the wake of greater awareness of the
problem and attention to dental hygiene before
and after initiating bisphosphonate therapy.
An American Academy of Oral Medicine position
paper on the management of bisphosphonaterelated ONJ (BONJ) was originally published in
The Journal of the American Dental Association in
December, 2005 and has been updated several
times, most recently in a 2014 position paper
entitled Medication-Related Osteonecrosis of the
Jaw – 2014 Update. The first recommendation is
prevention of medicine-related ONJ through regular dental check-ups. If a problem is found, referral to an expert (i.e., an oral surgeon) is strongly
However, additional concerns have emerged with
long-term used of bisphosphonates. Although
atypical (subtrochanteric) fractures of the femur
are rare, there is data that establishes an association with five or more years of bisphosphonate
treatment with their occurrence. In October 2010,
the FDA added subtrochanteric fracture of the
femur to the “Precautions and Warnings” section of
the package inserts for all bisphosphonates. Two
recent publications discuss the possible association
between oral bisphosphonates and cancer of the
Table 12. Tests Required To Monitor Therapy Responses
Blood Tests
• Routine blood counts
• Chemistry panel
• Liver function tests
• Myeloma protein measurements (serum protein electrophoresis plus quantitative immunoglobulins)
• Serum Free Light Chain Assays (Freelite®)
• Heavy/Light Chain Assay (Hevylite®)
• Serum β2 microglobulin
• C-reactive protein
• Peripheral blood labeling index (LI)
• Serum erythropoietin level
Urine
• Routine urinalysis
• 24-hour urine for measurement of total protein, electrophoresis, and immunoelectrophoresis
• 24-hour urine for creatinine clearance if serum creatinine elevated
Bone Evaluation
• Skeletal survey by X-ray
• MRI/CT scan for special problems
• Whole body FDG/PET scan if disease status unclear
• Bone density measurement (DEXA scan) as baseline and to assess benefit of bisphosphonates
Bone Marrow
• Aspiration and biopsy for diagnosis and periodic monitoring
• Special testing to assess prognosis looking for multiple potential karyotypic and FISH abnormalities
(number of chromosomes, translocations, deletions – e.g., FISH 13q-, t[4:14], 1q21, etc.)
Other Testing
• Amyloidosis
(special circumstances) • Neuropathy
• Renal or infectious complications
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esophagus. Using the same database, one group
did not find an association (Cardwell et al.), whereas
the other group reported an increased risk (Green
et al.). These findings require further examination.
The IMWG’s 2013 recommendations state that for
patients in CR or VGPR, the optimal duration of bisphosphonate therapy is not clear; bisphosphonates
should be administered for at least 12 months and
up to 24 months, and then at the physician’s discretion. For patients who have active disease, who
have not achieved a response, or who have threatening bone disease beyond two years, bisphosphonate therapy can be decreased to every three
months. The most current guidelines on the role
of bisphosphonates in myeloma from the American Society of Clinical Oncology (ASCO) (Kyle et al.
JCO 2007) recommend treating for two years, then
considering discontinuation of bisphosphonates
for patients whose disease is responsive or stable.
Continued use of bisphosphonates should be at
the discretion of the physician.
Antibiotics – Infections are a common and recurrent problem in patients with myeloma. A careful
strategy for infection management is required.
Antibiotic therapy should be instituted immediately if active infection is suspected. Use of preventative or prophylactic antibiotics with recurrent
infection is controversial. A comparative study
(URCC/ECOG, Vesole et al.) presented at ASH 2010
concluded that “the use of prophylactic antibiotics
did not decrease the incidence of serious infection (> grade 3 and/or hospitalization) nor of any
infection within the first 2 months of treatment.”
Based on this study, the authors recommend that
antibiotics should not be mandated in the first two
months of treatment, but should be considered on
a case-by-case basis. The continuation of prophylactic antibiotics can increase the chance of antibiotic resistance, but it can also reduce the chance of
recurrent infectious complications. The use of highdose gammaglobulin may be required in patients
with acute and severe recurrent infections. GM-CSF
may be helpful in improving the white blood cell
levels in an effort to overcome infectious complications. The use of G-CSF or GM-CSF is helpful in the
recovery phase following bone marrow or stem cell
transplantation. G-CSF and GM-CSF are also used in
harvesting stem cells.
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Antivirals – An increased incidence of herpes zoster (shingles) has been observed in some patient
populations with myeloma (but not other malignancies) who are treated with Velcade. Therefore,
prophylactic antiviral therapy should be considered with Velcade therapy. This has led to
the recommendation that patients receiving
carfilzomib, a second-generation proteasome
inhibitor, receive antiviral prophylaxis as well.
Myeloma patients are cautioned not to get the
shingles (Zostavax®) vaccine, as it is a live virus
that poses a significant risk to those who are
immune compromised.
Management of relapsing
or refractory disease
As illustrated in the pathophysiology section, a
frequent problem in myeloma is the relapse that
occurs following a 1- to 3-year remission. Although
maintenance therapy may be useful in prolonging the initial remission period, the relapse, which
supervenes inevitably, requires re-induction therapy. The following is an overall strategy for the
management of relapsing disease.
If first relapse occurs after a remission of at least
6 months to 1 year, the first strategy is to consider
re-utilizing the therapy that produced the remission in the first place. NCCN guidelines state that
“if the relapse occurs greater than 6 months after
completion of the initial primary therapy, patients
may be retreated with the same primary regimen.”
Approximately 50% of patients will experience a
second remission with the same therapy that produced the first. This is particularly true for patients
whose disease is in remission for more than one
year following the initial induction attempt. As
an example, a patient who received Revlimid/
low-dose dexamethasone and whose myeloma
has gone into remission for two years can again
receive Rd therapy. If remission has lasted less
than six months, some alternative therapy will
usually be required. This is also the case if relapse
has occurred following a second or third use of the
original induction therapy. Adding a third drug to
the regimen is an important consideration in this
setting. (See Figure 6.)
27
Figure 6. Multi-drug-resistant (MDR) myeloma cell
Velcade (bortezomib) for relapsing myeloma –
Velcade plays a crucial role as a platform on which
to base combination therapies for relapse (VR, VRD,
VCD, etc.). In August, 2014, based on the international Phase II RETRIEVE trial, Velcade was approved
in the US for the retreatment of adult patients with
myeloma who had previously responded to Velcade therapy and relapsed at least six months following completion of that therapy.
Kyprolis (carfilzomib) for relapsing myeloma –
Kyprolis has been evaluated alone and as a backbone drug in combination therapy trials for relapse
therapy. It has demonstrated safety and efficacy
in such combination therapies as KCyD, KRD, KTD,
and KCyTD, all of which were presented at ASH in
2012. Final results of the ASPIRE trial comparing
Kyprolis/Revlimid/dexamethasone to Revlimid/
dexamethasone in relapsed myeloma were presented at the 2014 annual ASH meeting, demonstrating the superiority of KRD over RD. Initial
results of the ENDEAVOR trial comparing Kyprolis/
dexamethasone to Velcade/dexamethasone in
myeloma patients who had had from one to three
prior therapies were released in March, 2015,
and demonstrated that patients who were in the
Kyprolis/dexamethasone arm had double the progression-free survival of patients in the Velcade/
dexamethasone arm (18.7 versus 9.4 months). Final
analysis of this trial, and of other trials going forward with Kyprolis, will have to determine whether
the higher-than-approved dose of Kyprolis in the
ENDEAVOR trial and the number of patients in the
trial who had had previous Velcade significantly
influenced the results. The results of the Kyprolis/
Pomalyst/dexamethasone trial in relapsed/refractory myeloma are not yet published at this time,
28
but preliminary data have shown a 75% overall
response rate with over 17 months progression-free
survival in highly pretreated patients.
Pomalyst has also demonstrated its value in the
relapse setting in multiple combination therapy
trials (PD, PVD, PCyPred, BiaxinPD, PCyD, KPD).
Encouraging recent news from the IFM was published in Blood in February 2015, indicating that
patients with early relapsed/refractory myeloma
who have high-risk deletions 17p and/or t(4;14)
show improved PFS and OS with Pomalyst/lowdose dexamethasone.
Other options – It is important to keep in mind that
a variety of single and combination chemotherapy
protocols are available for the management of
relapsing and refractory disease. Depending upon
the exact problem, a variety of interventions may
be possible. For example, if relapse is associated
with the development of one or two bone lesions,
radiation to the site(s) of bone involvement may
be a satisfactory way to manage the relapse. If
overall relapse has occurred, dexamethasone as a
single agent can be very useful in achieving overall
control of the disease. The use of dexamethasone
is attractive because it can be given by mouth and
does not cause significant side effects such as hair
loss or reduction in peripheral blood count values.
Another important point is that relapse following
high-dose therapy with transplant has, in many
cases, a pattern similar to relapse following more
standard approaches. Second and sometimes third
remissions can be achieved following relapse after
bone marrow transplantation. Whether a second
high-dose therapy with transplant is the most
appropriate strategy as opposed to some other
approach is currently unclear, and must be based
upon individual patient considerations.
Given the continuing rapid rate of development of
new therapies for myeloma, including second-generation proteasome inhibitors, third-generation
IMiDs, monoclonal antibodies, and targeted therapies, as well as investigation of new combinations
of existing and new agents, treatment in the context of clinical trials can be an option for patients
with relapsed myeloma.
800-452-CURE (2873)
A full range of supportive care is crucial for the
management of myeloma. When first diagnosed, a
number of emergency procedures may be required,
including dialysis, plasmapheresis, surgery, and
radiation to reduce pressure on a nerve, spinal
cord, or other crucial organ. The management of
pain is essential for the initial care of patients with
myeloma. This can be difficult until initial disease
control is achieved. There is no reason for patients
with myeloma to have major ongoing pain with the
range of new drugs and strategies available. There
can be reluctance on the part of the patient and/or
the physician to implement full pain control procedures because of concerns about addiction. Control
of pain should always be the first priority. A brace or
corset can help stabilize the spine or other areas,
reducing movement and pain. Moderate exercise
is also important in recovering bone strength and
mobility and can help in overall pain reduction.
New and emerging treatments
Most new treatments are available in the setting
of clinical trials. Clinical trial phases are listed in
Table 13. A whole range of agents is currently in
clinical trials, including oral proteasome inhibitors, monoclonal antibodies, histone deacetylase
(HDAC) inhibitors, tumor suppressor gene stimulators, chemotherapeutic agents, and therapies
targeted to myeloma-specific pathways. Patients
are encouraged to check with their physicians
regarding the availability of new clinical trials.
For questions or concerns, the IMF is available
via email at [email protected] or by calling
800-452-CURE (2873), toll-free in the United States
and Canada, or 818-487-7455 from other parts of
the world. The Myeloma Matrix, an IMF publication that lists all drugs currently in clinical trials for
myeloma, is available with regular updates in print
and with ongoing updates on the IMF website
myeloma.org. Good summaries of new therapies
are presented in the IMF reports from ASH, ASCO,
EHA, and IMWG. These summaries are available
online at myeloma.org or by calling the IMF.
myeloma.org
Table 13. Clinical Trial Phases
I
Early testing to assess dosing, tolerance, and toxicity
in patients
II
Further testing to evaluate how effective treatment is
at the dose and schedule selected
III
Comparison of the new treatment with prior treatment(s)
to determine if the new treatment is superior
Usually carried out after FDA approval to assess
IV cost-effectiveness, quality of life impact, and other
comparative issues
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800-452-CURE (2873)
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800-452-CURE (2873)
10 STEPS TO BETTER CARE®
A UNIQUE TOOL FOR DIAGNOSTIC
AND TREATMENT INFORMATION
One of the most daunting aspects of being diagnosed with multiple myeloma
(MM) is learning about – and understanding – an unfamiliar disease that is
quite complicated. From diagnosis to long-term survival, the 10 Steps to Better
Care® will guide you through the MM journey:
1. Know what you’re dealing with. Get the correct diagnosis.
2. Tests you really need.
3. Initial treatment options.
4. Supportive care and how to get it.
5. Transplant: Do you need one?
6. Response Assessment: Is treatment working?
7. Consolidation and/or maintenance.
8. Keeping Track of the Myeloma: Monitoring without mystery.
9. Relapse: Do you need a change in treatment?
10. New Trials: How to find them.
Visit 10steps.myeloma.org to gain a better understanding of the disease and
diagnosis, and proceed through the steps to learn the best tests, treatments,
supportive care, and clinical trials currently available.
As always, the International Myeloma Foundation (IMF) urges you to discuss all
medical issues thoroughly with your doctor. The IMF is here to equip you with
the tools to understand and better manage your MM. Visit the IMF website
myeloma.org or call the IMF InfoLine at 800-452-CURE (2873), which is staffed
by trained information specialists, with your questions or concerns. The IMF is
here to help.
Telephone:
800-452-CURE (2873)
(USA & Canada)
818-487-7455
(worldwide)
Fax: 818-487-7454
[email protected]
myeloma.org
Improving Lives Finding the Cure®
© 2015, International Myeloma Foundation, North Hollywood, California (cr_c4_15)
12650 Riverside Drive, Suite 206
North Hollywood, CA 91607 USA